多柔比星治疗软组织肉瘤患者在ANNOUNCE III期临床试验中的生活质量

IF 0.9 Q4 ONCOLOGY
B. V. Van Tine, A. Krarup-Hansen, L. Hess, A. A. Abdul Razak, V. Soldatenkova, Jennifer Wright, S. Park
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引用次数: 2

摘要

背景:建议在临床试验中常规收集患者报告的结局(PROs),包括与健康相关的生活质量,但肉瘤患者试验的数据有限。在这项分析中,汇总的PRO数据来自于参加了基于阿霉素的治疗的ANNOUNCE III期试验的晚期或转移性软组织肉瘤(STS)患者。方法:ANNOUNCE是一项III期试验,随机分配509名STS患者接受最多8个周期的阿霉素联合奥拉拉单抗或安慰剂治疗,随后接受单药奥拉拉单抗或安慰剂治疗。在任何治疗周期都允许使用右唑嗪。参与者在每个治疗周期完成欧洲癌症研究和治疗组织生活质量问卷-核心30 (EORTC QLQ-C30,评分为0-100)和简短疼痛量表短表修改(mBPI-sf,评分为0-10)。对纵向数据进行描述性分析,并通过接受阿霉素的累积剂量,为STS患者的临床护理提供信息。QLQ-C30的恶化被定义为在任何基线后评估中变化10分或更多。mPBI-sf恶化定义为较基线增加≥2点。结果:大多数参与者在试验期间完成了基线和至少一次后续PRO评估(n = 460, 90.4% EORTC QLQ-C30;n = 454, 89.2%, mBPI-sf)。参加ANNOUNCE试验的STS患者在开始使用阿霉素之前,存在有临床意义的身体功能和疼痛问题。总的来说,那些在基线时症状较少或功能较好的患者在整个研究过程中接受了较高的累积阿霉素剂量。基线时,QLQ-C30疲劳平均为29.9分,至首次恶化的中位时间为0.9个月;恶心/呕吐平均为6.5分,至恶化的平均时间为1.4个月;平均身体机能为78.3,中位恶化时间为2.1个月;平均健康状况为66.8,中位首次恶化时间为1.6个月。疼痛恶化的中位时间为7.9个月。结论:晚期或转移性肉瘤患者报告说,在以阿霉素为基础的治疗期间,PROs下降相对迅速,患者在基线时症状较差(特别是疲劳),随后接受较少的阿霉素治疗。在阿霉素治疗期间,从患者角度获得详细的汇总数据,可以为这些患者的未来护理提供信息,并可以为未来试验中PRO终点的开发提供资源。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Quality of life of patients with soft tissue sarcoma treated with doxorubicin in the ANNOUNCE phase III clinical trial
Background: Patient-reported outcomes (PROs), including health-related quality of life, are recommended to be routinely collected in clinical trials, but data are limited from trials of sarcoma patients. In this analysis, pooled PRO data are reported from patients with advanced or metastatic soft tissue sarcoma (STS) enrolled to the ANNOUNCE phase III trial of doxorubicin-based therapy. Methods: ANNOUNCE was a phase III trial that randomized 509 patients with STS to receive up to eight cycles of doxorubicin with olaratumab or placebo, followed by single-agent olaratumab or placebo. Dexrazoxane was allowed at any cycle of treatment. Participants completed the European Organization for Research and Treatment of Cancer Quality of Life Questionnaire-Core 30 (EORTC QLQ-C30, which is scored 0–100), and Brief Pain Inventory Short Form Modified (mBPI-sf, scored from 0–10) at each treatment cycle. A descriptive analysis of the longitudinal data was conducted overall and by cumulative dose of doxorubicin received to inform the clinical care of patients with STS. Worsening on the QLQ-C30 was defined as a change of 10 points or more at any post-baseline assessment. Worsening on the mPBI-sf was defined as an increase of ≥2 points from baseline. Results: The majority of participants completed the baseline and at least one subsequent PRO assessment within the trial (n = 460, 90.4% EORTC QLQ-C30; n = 454, 89.2%, mBPI-sf). Patients with STS enrolled to the ANNOUNCE trial had clinically meaningful problems with physical function and pain before initiating doxorubicin. Overall, those with fewer symptoms or better function at baseline received higher cumulative doxorubicin dose throughout the study. At baseline, mean QLQ-C30 fatigue was 29.9 with a median time to first worsening of 0.9 months, and mean nausea/vomiting was 6.5 with 1.4 months until worsening; mean physical function was 78.3 with median time to worsening of 2.1 months and mean health status was 66.8 with median time to first worsening of 1.6 months. Median time to worsening of pain was 7.9 months. Conclusion: Patients with advanced or metastatic sarcoma reported a relatively rapid decline in PROs during doxorubicin-based treatment, with patients with poorer symptoms at baseline (specifically fatigue), subsequently receiving less doxorubicin therapy. The availability of detailed summary data from the patient perspective during doxorubicin-based treatment may inform future care of these patients and can provide a resource for the development of PRO endpoints in future trials.
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Rare Tumors
Rare Tumors ONCOLOGY-
CiteScore
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